EP0692717B1 - Analysis instrument - Google Patents

Analysis instrument Download PDF

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Publication number
EP0692717B1
EP0692717B1 EP95110802A EP95110802A EP0692717B1 EP 0692717 B1 EP0692717 B1 EP 0692717B1 EP 95110802 A EP95110802 A EP 95110802A EP 95110802 A EP95110802 A EP 95110802A EP 0692717 B1 EP0692717 B1 EP 0692717B1
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EP
European Patent Office
Prior art keywords
probe
gross
predetermined
liquid
fine
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Expired - Lifetime
Application number
EP95110802A
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German (de)
French (fr)
Other versions
EP0692717A3 (en
EP0692717A2 (en
Inventor
Keith Aldan Ely
Robert Eric Bernstine
Timothy Patrick Evers
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Dade Chemistry Systems Inc
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Dade Chemistry Systems Inc
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Publication date
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Publication of EP0692717A2 publication Critical patent/EP0692717A2/en
Publication of EP0692717A3 publication Critical patent/EP0692717A3/en
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Publication of EP0692717B1 publication Critical patent/EP0692717B1/en
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    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1081Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices characterised by the means for relatively moving the transfer device and the containers in an horizontal plane
    • G01N35/1083Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices characterised by the means for relatively moving the transfer device and the containers in an horizontal plane with one horizontal degree of freedom
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/02Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor using a plurality of sample containers moved by a conveyor system past one or more treatment or analysis stations
    • G01N35/04Details of the conveyor system
    • G01N2035/0439Rotary sample carriers, i.e. carousels
    • G01N2035/0441Rotary sample carriers, i.e. carousels for samples
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1065Multiple transfer devices
    • G01N2035/1076Multiple transfer devices plurality or independently movable heads
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1081Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices characterised by the means for relatively moving the transfer device and the containers in an horizontal plane
    • G01N35/1083Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices characterised by the means for relatively moving the transfer device and the containers in an horizontal plane with one horizontal degree of freedom
    • G01N2035/1086Cylindrical, e.g. variable angle
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/02Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor using a plurality of sample containers moved by a conveyor system past one or more treatment or analysis stations
    • G01N35/025Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor using a plurality of sample containers moved by a conveyor system past one or more treatment or analysis stations having a carousel or turntable for reaction cells or cuvettes
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1004Cleaning sample transfer devices

Definitions

  • the present invention relates to a chemical analysis instrument, and in particular, to a chemical analysis instrument wherein both a gross probe and a fine probe are movable along independent loci of action among various analysis, treatment and/or other liquid handling devices.
  • An open container presents no obstacle to the withdrawal of a precisely metered volume of a sample for analysis.
  • Complications are encountered with the use of an evacuated capped container.
  • One complication is the need of a relative more substantial sample probe to penetrate the rubber stopper. Such a sampling probe may not be able to meter precisely relatively small amounts of liquid.
  • a further complication is the difficulty to extract accurately a predetermined volume of sample due to air pressure within the tube. The tube may be vented before a sample may be withdrawn.
  • any pre-analysis treatment of the extracted sample be handled in an efficient manner.
  • Such pretreatment may include dilution or stabilization.
  • the sample must be efficiently routed to the appropriate analysis device(s) for appropriate chemical analysis.
  • US-A-4,721,137 has a puncture tube which first penetrates the stopper and a sampling probe which is separate from the puncture tool to extract a liquid sample.
  • US-A-4,577,514 and US-A-4,622,475 both have a puncture tube which first penetrates the stopper and a separate sampling probe which is movable concentrically within the puncture tube to extract a liquid sample.
  • US-A-4,951,512 uses a puncture tube to create an opening in the closed cap of the container and either takes a sample through this puncture tube or inserts a separate probe through the puncture tube to measure properties of the sample.
  • US-A-4,756,201 and US-A-5,201,232 both disclose an apparatus that extracts samples from open and closed containers.
  • these apparatus both require that a closed tube be segregated by an operator and positioned upside-down for sampling to occur. This renders automation difficult since open tubes must be positioned apart from and handled differently from the closed tubes.
  • US-A-5,216,926 provides an apparatus for sampling from both open and closed containers.
  • the disclosed apparatus includes a single transfer vessel to contain extracted samples.
  • US-A-4,774,055 discloses an open tube analysis instrument in which three separate pipettes are provided.
  • One pipette extracts sample from a sample support table and deposits it in a reaction chamber disposed on a rotatable table.
  • the other two pipettes dispense reagent into the reaction chamber.
  • the rotatable table carrying the sample chamber is coaxial with the sample support table.
  • US 5 296 911 discloses an optical test system for chemical analyzer which has a support for supporting open containers for samples and a movable probe which extracts liquid from the containers and moves the liquid to a rotating carrier having a plurality of liquid receiving wells. After the liquid is dispensed by the probe into the wells of the carrier, the carrier rotates to supply the liquid to the optical test system.
  • This chemical analyzer does not allow for a flexible operation, like for example testing of two liquids in one process, or subsequent testing of one liquid.
  • EP-A-0 252 631 shows a modular analyzer system which has a rotating support for containers which can be used by more than one analyzer system.
  • this modular analyzer system no distinction is made between a gross probe and a fine probe which means that no analysis having subsequent testing steps like a gross and a fine testing step can be performed.
  • an analysis instrument having such flexibility of operation as to permit sample extracted from either capped or open containers to be dispensed to any one of a plurality of predetermined locations, including one or more analysis device(s), with or without the benefit or dilution of other forms of pre-treatment.
  • An analysis instrument in accordance with the present invention includes a support (12) for supporting closed or open sample liquid containers (T c , T o ), a gross probe (40), a fine probe (50), and a carrier (24) having a plurality of liquid receiving wells (24W).
  • the probes (40, 50) are each able either to dispense or to draw (extract) a volume of liquid sample or other liquid.
  • the support (12) is movable to dispose any one of the containers (T c , T o ) at either a gross probe sample extracting position (18I, 18E) or at a fine probe sample extracting position (20I, 20E), while the carrier (24) is movable to dispose any one of the plurality of liquid receiving wells (24W) therein at either a gross probe dispensing position (28I, 28E) or a fine probe operating position (30I, 30E).
  • the gross probe (40) is movable along a locus of action (42) between the gross probe sample extracting position (18I, 18E) and the gross probe dispensing position (28I, 28E).
  • the gross probe sample extracting position (18I, 18E) the gross probe (40) is able to draw thereinto liquid sample from either a closed or an open container (T c , T o ) there disposed by the support (12).
  • the gross probe dispensing position (28I, 28E) the gross probe is able to dispense previously withdrawn liquid into a well (24W) there disposed by the carrier (24).
  • the fine probe (50) is movable along a locus of action (52) between a fine probe sample extracting position (20I, 20E) and a fine probe operating position (30I, 30E).
  • a fine probe sample extracting position (20I, 20E) the fine probe (50) is able to draw thereinto liquid sample from an open container (T o ) there disposed by the support (12), while in the fine probe operating position (30I, 30E) the fine probe is able either to dispense therefrom previously withdrawn liquid or to draw thereinto liquid, both from a well (24W) there disposed by the carrier (24).
  • An analysis instrument (70) may be disposed at a position (74) located along the locus of action (52) of the fine probe (50). Additionally, a reservoir (58) holding a sample treatment liquid may be disposed at a second extracting position (64) located along the locus of action (42) of the gross probe (40) and a reservoir (72) holding a sample treatment liquid may be disposed at a second extracting position (76) located along the locus of action (52) of the fine probe (50).
  • the various sample analysis, sample treatment and/or sample handling devices are arranged so that both the gross probe (40) and the fine probe (50) are each independently movable along their respective loci of action (42, 52) among one or more various extracting position(s), one or more various dispensing position(s), and/or one or more various operating position(s) (i. e., positions where either extracting and/or dispensing may occur), thus imparting a flexibility of operation to the instrument (10) so configured.
  • the Figure schematically illustrates a portion of an analysis instrument, generally indicated by the reference character 10, the various sample analysis, liquid handling, and sample treatment devices thereof being relatively positioned with respect to each other in a predetermined manner in accordance with the invention. Since the Figure is intended as a schematic illustration, details regarding particular structural details of the instrument, such as the instrument framework and housing, and the manner in which various of the devices are interconnected to their associated drive actuator, and overall operating controller, are omitted. However, these and other details should be readily apparent to those skilled in the art, especially in view of commercially available analysis instruments of the same general type. Exemplary of such commercially available instruments is the clinical chemistry system manufactured and sold by the Medical Products Division of E. I. du Pont de Nemours and Company under the trademark Dimension®.
  • the instrument 10 includes a sample container support 12 for supporting closed or open containers, each having a liquid therein.
  • the liquid may be a sample of a patient's body liquid, a calibrator liquid, or a chemical reagent liquid.
  • T c Several of the closed containers are generally indicated in various slots by the reference character T c , while representative open containers are generally indicated by the reference character To.
  • the container support 12 is preferably implemented in the form of a generally circular wheel 12.
  • the support 12 may be shaped other than circularly, if desired.
  • the support 12 is preferably rotatably movable with respect to an axis 12A. It should be understood that the support 12 may, alternately, be movable in direction(s) other than rotatably.
  • the support 12 may be rectilinearly movable with respect to the axis 12A along one or more directions, some of which may be mutually perpendicular if desired.
  • the wheel 12 includes an annular, hollowed rim 14 that is generally U-shaped in cross section bounded by radially inner and outer rails 14R.
  • a plurality of arcutely shaped sample trays 16 is received by rim 14.
  • Each sample tray 16 is held radially in place by the rails 14R.
  • Each tray 16 has one or more arcuate rows of sample container receiving slots 16S.
  • Each slot 16S is appropriately sized and configured to receive either an open container T o or a closed container T c therein.
  • Each row of slots 16S in each segment 16 cooperates with the corresponding row of slots 16S in the angularly adjacent segment to define at least one annular array, but more preferably, both an inner and an outer concentric annular array of slots.
  • the inner array of slots is indicated by the reference character 16A, while the outer array of slots is indicated by the character 16B. It should also be understood that the slots may be otherwise arrayed, as in a spiral pattern, and remain within the contemplation of this invention.
  • the container support 12 is operatively connected to a suitable actuator (diagrammatically indicated by the reference character A S ) for effecting the desired movement thereof with respect to the axis 12A.
  • a suitable actuator (diagrammatically indicated by the reference character A S ) for effecting the desired movement thereof with respect to the axis 12A.
  • Suitable for use as the actuator A S is an encoded stepper motor driven belt.
  • the support 12 is movable to dispose any one of the containers received within a slot 16S in the slot array to at least two predetermined sample extracting positions defined at predetermined spaced locations with respect to the axis 12A.
  • rotatable movement of the support 12 serves to position any container T c , T o carried in a slot 16S in the inner concentric annular array 16A to at least either a first predetermined inner sample extracting position 18I or a second predetermined inner sample extracting position 20I.
  • movement of the support 12 by the actuator A S serves to position any container T c , T o carried in a slot 16S in the outer concentric annular array 16B to at least either a first predetermined outer sample extracting position 18E or a second predetermined outer sample extracting position 20E.
  • the sample extracting positions 18I, 18E, respectively, and the sample extracting positions 20I, 20E, respectively, are angularly offset from each other by predetermined angular distances.
  • each tray 16 may have one or more arcuate row(s) of sample container receiving slots disposed between the radially inner and outer rows shown in the Figure. Such additional arcuate rows would cooperate to define additional intermediate concentric annular array(s) of slots.
  • a pair of predetermined sample extracting positions is defined for each additional annular array.
  • a slot in each additional annular array may be positioned at either sample extracting position in the pair by movement of the support 12.
  • T o in a slot 16S in any particular annular array (e. g., 16A, 16B)is positioned at either of the inner sample extracting positions 18I, 20I or at either of the outer sample extracting positions 18E, 20E corresponding to that array, the liquid therein is able to be withdrawn therefrom.
  • the instrument 10 also includes a carrier 24 having a plurality of liquid receiving wells 24W therein formed to define at least one generally annular array 26.
  • the carrier 24 has at least both an inner and an outer concentric annular array 26A, 26B, respectively, of wells 24W.
  • Each well 24W is sized to accommodate at least a predetermined liquid volume, and thus defines a receptacle wherein sample liquid may be handled and treated.
  • the carrier 24 is operatively connected to a suitable actuator (diagrammatically indicated by the reference character A c , similar to the actuator A S ) whereby the carrier 24 is movable with respect to an axis 24A.
  • the axis 24A is displaced from the axis 12A of the container support 12.
  • the carrier 24 is rotatably moved with respect to the axis 24A.
  • the carrier 24 may be otherwise movable, as in one or more rectilinear directions, some of which may be mutually perpendicular.
  • the carrier 24 is movable with respect to the axis 24A to dispose any of the wells 24W at one or more predetermined positions.
  • appropriate rotatable movement of the carrier 24 with respect to the axis 24A serves to dispose any one of the wells 24W in each annular array to at least two predetermined operating positions defined at predetermined spaced angular locations with respect to the axis 24A.
  • the wells 24W may also be otherwise arrayed, e.g., in a spiral pattern. Although shown as circular in shape in the Figure, it should be understood that the carrier 24 may exhibit any desired shape.
  • rotatable movement of the carrier 24 serves to position any well 24W disposed in the inner concentric circular array 26A to at least either a first predetermined inner operating position 28I or an angularly offset second predetermined inner operating position 30I.
  • movement of the carrier 24 by the actuator A c serves to position any well 24W disposed in the outer concentric circular array 26B to at least either a first predetermined outer operating position 28E or an angularly offset second predetermined outer operating position 30E.
  • the carrier 24 may have one or more additional annular array(s) of wells disposed between the radially inner and outer arrays of wells shown in the Figure. At least two predetermined operating positions are defined for a well in each additional annular array of wells. As will be developed when a well 24W is disposed at a given operating position a liquid may be either drawn therefrom (i. e., extracted therefrom) and/or dispensed thereinto.
  • the instrument 10 further includes sample handling devices in the form of a first, gross, probe 40 and a second, fine, probe 50.
  • the gross probe 40 is operatively connected to an actuator (diagrammatically indicated by the reference character A g ) whereby the probe 40 is movable along a predetermined, preferably circular, locus 42 centered about an axis 40A.
  • the axis 40A is spaced with respect to the axes 12A and 24A of the support 12 and the carrier 24, respectively.
  • the actuator A g is implemented in the form of a belt driven by an encoded stepping motor.
  • the fine probe 50 is operatively connected to an actuator (diagrammatically indicated by the reference character A f , similar to the actuator A g ) whereby the probe 50 is movable along a separate predetermined locus 52.
  • the locus 52 is centered about an axis 50A that is spaced with respect to the axes 12A and 24A of the support 12 and the carrier 24, respectively, and with respect to the axis 40A of the probe 40.
  • the locus 52 of the fine probe 50 is also preferably generally circular in form.
  • the gross probe 40 may be implemented by any suitable liquid extracting arrangement so long as the probe 40 is able to draw (i. e., extract) liquid from either a closed or an open tube or other liquid reservoir or liquid receptacle. To satisfy the needs of the present invention the gross probe 40 is required only to be able to control in a relatively gross manner the volume of liquid able to be either drawn thereinto or dispensed therefrom.
  • the term "relatively gross control" should be construed to mean liquid volume control to the order of ten microliters. Details of the preferred form of the liquid extraction apparatus used to implement the gross probe are disclosed and claimed in above referenced contemporaneously filed copending application, assigned to the assignee of this invention.
  • the fine probe 50 is required to be able to draw or to dispense relatively finely metered amounts of liquid.
  • the term "relatively finely metered” should be construed to mean liquid volume control to the order of tenths of microliters.
  • the locus 42 of the gross probe 40 contains the first predetermined inner sample extracting position 18I, the first predetermined outer sample extracting position 18E, the first predetermined inner operating position 28I, and the first predetermined outer operating position 28E.
  • the gross probe When positioned at either the inner sample extracting position 18I or the outer sample extracting position 18E the gross probe is able to draw thereinto liquid sample that is carried within either a closed container T c or an open container T o that is disposed by the support 12 at that sample extracting position.
  • the gross probe is able either to dispense into the well 24W positioned at the position 28I, 28E liquid that has been previously drawn into the probe or to draw into the probe (i. e., extract from the well) liquid that is present in the well.
  • the locus 52 of the fine probe 50 contains the first predetermined inner sample extracting position 20I, the first predetermined outer sample extracting position 20E, the first predetermined inner operating position 30I, and the first predetermined outer operating position 30E.
  • the fine probe 50 When positioned at either the inner sample extracting position 20I or the outer sample extracting position 20E the fine probe 50 is able to draw thereinto liquid sample that is carried within an open container T o that is disposed by the support 12 at that sample extracting position.
  • the fine probe is able either to dispense into the well positioned at the position 30I, 30E liquid that has been previously drawn into the probe or to draw into the fine probe (i. e., extract from the well) liquid that is present in the well.
  • Various other liquid handling, sample analysis and/or sample treatment functional devices of the analysis instrument 10 may be positioned about the locus 42 defined by the movement of the gross probe 42.
  • three such representative additional devices 56, 58, 60 are respectively located at predetermined angular positions 62, 64, 66 along the locus 42.
  • each of these angular positions 62, 64, 66 defines an operating position at which the gross probe is able either to dispense liquid or to extract liquid.
  • the precise function of the device 56, 58, 60 at each respective angular position 62, 64, 66 will serve to determine the primary action performed by the probe at a given location.
  • the device 56 located at the angular position 62 is, in the preferred implementation of the instrument 10, an analysis device of the ion selective electrode (ISE) type.
  • ISE ion selective electrode
  • Suitable for use as the ion selective electrode analysis device is that device manufactured by the Medical Products division of E. I. du Pont de Nemours and Company as sold as part of the clinical chemistry system identified by the trademark Dimension®. This analysis device is disclosed in United States Patent 5,284,568 issued on February 8, 1994 and assigned to the assignee of the present invention.
  • the primary action of the probe 40 at the analysis device 56 is the dispensation of liquid sample or treated sample from the probe into the analysis device. Accordingly, the angular location 62 serves to define a second dispensing position along the locus 42 at which the probe 40 may dispense liquid.
  • the device 58 located at the angular position 64 is, in the preferred implementation of the instrument 10, a liquid reservoir for either a treatment liquid, (e. g., a diluent liquid solution for diluting a patient sample or a chemical reagent for chemically treating the patient sample) or a wash station for cleaning the liquid handling probe.
  • a treatment liquid e. g., a diluent liquid solution for diluting a patient sample or a chemical reagent for chemically treating the patient sample
  • a wash station for cleaning the liquid handling probe.
  • the primary action of the probe 50 at the device 58 is extracting liquid from the reservoir into the probe.
  • the angular location 62 would serve to define a second liquid extracting position along the locus 42 at which the probe may draw a liquid thereinto.
  • the latter case i.
  • the device 58 disposed in the position 64 may be either a reservoir or a drain, dependent upon the form of probe wash utilized. If the wash liquid is disposed in a reservoir, then the primary actions of the probe 50 at the device 58 would include both dispensing liquid to and extracting liquid from the reservoir. However, if the wash liquid is pumped into and through the probe from a source (not shown) then the primary action of the probe 50 at the device 58 would be the dispensing of liquid into the drain. Thus at the wash location the probe 50 may either extract, dispense, or both, as appropriate.
  • a diluent or a reagent liquid solution is disposed in the reservoir 58, then it lies within the contemplation of the invention to dispose the wash solution in a second reservoir device 60 which may be disposed at the angular position 66. Since at a wash position the probe both dispenses and extracts, the angular position 66 would serve to define a third extracting position at which the probe 40 draws liquid thereinto.
  • additional liquid handling, sample analysis and/or sample treatment functional devices such as additional reservoir(s) for other chemical liquids may also be positioned at additional location(s) about the locus 42, e.g., a reservoir 58A at an angular position 64A may contain a liquid chemical reagent.
  • various additional functional devices of the analysis instrument 10 may be positioned about the locus 52 defined by the movement of the fine probe 50.
  • two such additional devices 70, 72 are respectively located at respective predetermined angular positions 74, 76 along the locus 52.
  • each of these angular positions 74, 76 defines an operating position at which the gross probe is able either to dispense liquid or to extract liquid.
  • the precise function of the device 70, 72 at the respective angular position 74, 76 will serve to determine the primary action performed by the probe 50 at a given location.
  • the device 70 located at the angular position 74 is, in the preferred implementation of the instrument 10, an analysis device of the photometric type. Suitable for use as the photometric analysis device is that manufactured and sold by the Medical Products division of E. I. du Pont de Nemours and Company as part of the clinical chemistry system identified by the trademark Dimension®. This photometric analysis is disclosed in United States Patent 4,863,693 issued on September 5, 1989 to G. W. Howell and assigned to the assignee of the present invention.
  • the primary action of the probe 50 at the analysis device 70 is the dispensation of liquid from the probe into the analysis device. Accordingly, with respect to the fine probe 50, the angular location 74 serves to define a second dispensing position along the locus 52 at which the probe 50 may dispense liquid.
  • the device 72 located at the angular position 76 is, in the preferred implementation of the instrument 10, a liquid reservoir, primarily for a wash solution. Noting that at a wash position the probe 50 both dispenses and extracts liquid, the angular position 76 serves to define a second liquid extracting position along the locus 52 of the probe 50. In keeping with the foregoing it should be appreciated that additional devices of various functionality may be additionally disposed at spaced angular positions along the locus 52.
  • both the probe 40 and the probe 50 are each independently movable along their respective loci of action 42, 52 among one or more various extracting position(s), one or more various dispensing position(s) and/or one or more various operating position(s) (i. e., both extracting and dispensing).
  • the flexibility of operation imparted to an instrument 10 so configured may be made more clear from the following operational examples.
  • slots 16S1, 16S2 and 16S6 Three closed containers are positioned in slots 16S1, 16S2 and 16S6, the containers indicated by reference characters T c1 , T c2 and T c6 , respectively.
  • Three open containers are positioned in slots 16S3, 16S4 and 16S5, the containers indicated by reference characters T o3 , T o4 , T o5 , respectively.
  • Slots 16S1 and 16S3 are located on the outcr concentric circular array 16B.
  • Slots 16S2 and 16S4 are located on the inner concentric circular array 16A, respectively.
  • Slots 16S5 and 16S6 are located on the outer concentric circular array 16B.
  • Analytical Test 1 in which a liquid sample is extracted from a closed container and provided to two separate analysis devices without pretreatment.
  • Analytical test 2 in which liquid sample is extracted from a closed container and provided to a first analysis device without pretreatment and is also provided to a second analysis device after a diluting pretreatment.
  • Analytical Test 3 in which a liquid sample is extracted from an open container and provided to two separate analysis instruments without pretreatment.
  • Analytical Test 4 in which a liquid sample is extracted from a closed container and provided to a first analysis device after pretreatment and is also provided to a second analysis device before and after a diluting pretreatment.
  • Analytical Test 5 in which a first liquid sample is extracted from an open container and provided directly to a first analysis device without pretreatment and in which a second liquid sample is extracted from an open container and provided directly to a second analysis device without pretreatment.
  • Analytical Test 6 in which liquid samples extracted from closed and open containers are provided to an analysis device(s) in a different sequence than that in which they were extracted from the containers without pretreatment.
  • Analytical Test 7 in which a liquid sample is extracted from a closed container and provided to a second analysis device after a diluting pretreatment and after a chemical reagent pretreatment.

Description

  • The present invention relates to a chemical analysis instrument, and in particular, to a chemical analysis instrument wherein both a gross probe and a fine probe are movable along independent loci of action among various analysis, treatment and/or other liquid handling devices.
  • In the field of automatic analytical and diagnostic analysis there is a premium placed on the ability of an instrument to exhibit a high throughput, that is, the ability to process a relatively large number of patient samples in a given period of time. Samples which are non-toxic and non-hazardous are carried in open containers, such as open test tubes. However, to avoid exposing operators to contact with potentially hazardous serum and other unsafe materials, it may be desirable to carry other samples in containers which are capped, i. e., the top of the container is closed by a rubber stopper or other suitable cap mechanism. Exemplary of a closed container is that container sold by Becton-Dickinson Company, East Rutherford, New Jersey, under the trademark Vacutainer®. Such a container is evacuated to facilitate aspiration of a whole blood sample from a patient.
  • It is necessary in the context of automated high throughput analysis instrument to be able to provide a precise amount of an extracted sample from either an open or closed container. An open container presents no obstacle to the withdrawal of a precisely metered volume of a sample for analysis. Complications are encountered with the use of an evacuated capped container. One complication is the need of a relative more substantial sample probe to penetrate the rubber stopper. Such a sampling probe may not be able to meter precisely relatively small amounts of liquid. A further complication is the difficulty to extract accurately a predetermined volume of sample due to air pressure within the tube. The tube may be vented before a sample may be withdrawn.
  • In addition to being able to sample from both open and closed tubes, to effectuate high throughput it is imperative that any pre-analysis treatment of the extracted sample be handled in an efficient manner. Such pretreatment may include dilution or stabilization. Thereafter, the sample must be efficiently routed to the appropriate analysis device(s) for appropriate chemical analysis. These steps be performed without the necessity of any operator intervention and with apparatus having the minimum necessary mechanical complexity.
  • US-A-4,721,137 has a puncture tube which first penetrates the stopper and a sampling probe which is separate from the puncture tool to extract a liquid sample. US-A-4,577,514 and US-A-4,622,475 both have a puncture tube which first penetrates the stopper and a separate sampling probe which is movable concentrically within the puncture tube to extract a liquid sample. US-A-4,951,512 uses a puncture tube to create an opening in the closed cap of the container and either takes a sample through this puncture tube or inserts a separate probe through the puncture tube to measure properties of the sample.
  • US-A-4,756,201 and US-A-5,201,232 both disclose an apparatus that extracts samples from open and closed containers. However, these apparatus both require that a closed tube be segregated by an operator and positioned upside-down for sampling to occur. This renders automation difficult since open tubes must be positioned apart from and handled differently from the closed tubes.
  • US-A-5,216,926 provides an apparatus for sampling from both open and closed containers. The disclosed apparatus includes a single transfer vessel to contain extracted samples.
  • US-A-4,774,055 discloses an open tube analysis instrument in which three separate pipettes are provided. One pipette extracts sample from a sample support table and deposits it in a reaction chamber disposed on a rotatable table. The other two pipettes dispense reagent into the reaction chamber. The rotatable table carrying the sample chamber is coaxial with the sample support table.
  • US 5 296 911 discloses an optical test system for chemical analyzer which has a support for supporting open containers for samples and a movable probe which extracts liquid from the containers and moves the liquid to a rotating carrier having a plurality of liquid receiving wells. After the liquid is dispensed by the probe into the wells of the carrier, the carrier rotates to supply the liquid to the optical test system. This chemical analyzer does not allow for a flexible operation, like for example testing of two liquids in one process, or subsequent testing of one liquid.
  • EP-A-0 252 631 shows a modular analyzer system which has a rotating support for containers which can be used by more than one analyzer system. In this modular analyzer system, no distinction is made between a gross probe and a fine probe which means that no analysis having subsequent testing steps like a gross and a fine testing step can be performed.
  • In view of the foregoing it is believed advantageous to provide an analysis instrument having such flexibility of operation as to permit sample extracted from either capped or open containers to be dispensed to any one of a plurality of predetermined locations, including one or more analysis device(s), with or without the benefit or dilution of other forms of pre-treatment.
  • This problem is solved, according to the invention, with the features of claim 1.
  • An analysis instrument in accordance with the present invention includes a support (12) for supporting closed or open sample liquid containers (Tc, To), a gross probe (40), a fine probe (50), and a carrier (24) having a plurality of liquid receiving wells (24W). The probes (40, 50) are each able either to dispense or to draw (extract) a volume of liquid sample or other liquid. The support (12) is movable to dispose any one of the containers (Tc, To) at either a gross probe sample extracting position (18I, 18E) or at a fine probe sample extracting position (20I, 20E), while the carrier (24) is movable to dispose any one of the plurality of liquid receiving wells (24W) therein at either a gross probe dispensing position (28I, 28E) or a fine probe operating position (30I, 30E).
  • The gross probe (40) is movable along a locus of action (42) between the gross probe sample extracting position (18I, 18E) and the gross probe dispensing position (28I, 28E). In the gross probe sample extracting position (18I, 18E) the gross probe (40) is able to draw thereinto liquid sample from either a closed or an open container (Tc, To) there disposed by the support (12). In the gross probe dispensing position (28I, 28E) the gross probe is able to dispense previously withdrawn liquid into a well (24W) there disposed by the carrier (24).
  • The fine probe (50) is movable along a locus of action (52) between a fine probe sample extracting position (20I, 20E) and a fine probe operating position (30I, 30E). In the fine probe sample extracting position (20I, 20E) the fine probe (50) is able to draw thereinto liquid sample from an open container (To) there disposed by the support (12), while in the fine probe operating position (30I, 30E) the fine probe is able either to dispense therefrom previously withdrawn liquid or to draw thereinto liquid, both from a well (24W) there disposed by the carrier (24).
  • An analysis instrument (70) may be disposed at a position (74) located along the locus of action (52) of the fine probe (50). Additionally, a reservoir (58) holding a sample treatment liquid may be disposed at a second extracting position (64) located along the locus of action (42) of the gross probe (40) and a reservoir (72) holding a sample treatment liquid may be disposed at a second extracting position (76) located along the locus of action (52) of the fine probe (50).
  • In general, the various sample analysis, sample treatment and/or sample handling devices are arranged so that both the gross probe (40) and the fine probe (50) are each independently movable along their respective loci of action (42, 52) among one or more various extracting position(s), one or more various dispensing position(s), and/or one or more various operating position(s) (i. e., positions where either extracting and/or dispensing may occur), thus imparting a flexibility of operation to the instrument (10) so configured.
  • The invention will be more fully understood from the following detailed description, taken in connection with the accompanying drawing, which forms part of this application, and in which:
       the sole Figure is a schematic plan view of a portion of an analysis instrument in accordance with the present invention wherein the various sample analysis, sample handling and sample treatment devices are relatively positioned in a predetermined arrangement.
  • The Figure schematically illustrates a portion of an analysis instrument, generally indicated by the reference character 10, the various sample analysis, liquid handling, and sample treatment devices thereof being relatively positioned with respect to each other in a predetermined manner in accordance with the invention. Since the Figure is intended as a schematic illustration, details regarding particular structural details of the instrument, such as the instrument framework and housing, and the manner in which various of the devices are interconnected to their associated drive actuator, and overall operating controller, are omitted. However, these and other details should be readily apparent to those skilled in the art, especially in view of commercially available analysis instruments of the same general type. Exemplary of such commercially available instruments is the clinical chemistry system manufactured and sold by the Medical Products Division of E. I. du Pont de Nemours and Company under the trademark Dimension®.
  • The instrument 10 includes a sample container support 12 for supporting closed or open containers, each having a liquid therein. The liquid may be a sample of a patient's body liquid, a calibrator liquid, or a chemical reagent liquid. Several of the closed containers are generally indicated in various slots by the reference character Tc, while representative open containers are generally indicated by the reference character To. The container support 12 is preferably implemented in the form of a generally circular wheel 12. The support 12 may be shaped other than circularly, if desired. The support 12 is preferably rotatably movable with respect to an axis 12A. It should be understood that the support 12 may, alternately, be movable in direction(s) other than rotatably. For example, the support 12 may be rectilinearly movable with respect to the axis 12A along one or more directions, some of which may be mutually perpendicular if desired. The wheel 12 includes an annular, hollowed rim 14 that is generally U-shaped in cross section bounded by radially inner and outer rails 14R. A plurality of arcutely shaped sample trays 16 is received by rim 14. Each sample tray 16 is held radially in place by the rails 14R. Each tray 16 has one or more arcuate rows of sample container receiving slots 16S. Each slot 16S is appropriately sized and configured to receive either an open container To or a closed container Tc therein. Each row of slots 16S in each segment 16 cooperates with the corresponding row of slots 16S in the angularly adjacent segment to define at least one annular array, but more preferably, both an inner and an outer concentric annular array of slots. The inner array of slots is indicated by the reference character 16A, while the outer array of slots is indicated by the character 16B. It should also be understood that the slots may be otherwise arrayed, as in a spiral pattern, and remain within the contemplation of this invention.
  • The container support 12 is operatively connected to a suitable actuator (diagrammatically indicated by the reference character AS) for effecting the desired movement thereof with respect to the axis 12A. Suitable for use as the actuator AS is an encoded stepper motor driven belt. In general, the support 12 is movable to dispose any one of the containers received within a slot 16S in the slot array to at least two predetermined sample extracting positions defined at predetermined spaced locations with respect to the axis 12A. More particularly, in the context of the double concentric annular array arrangement of the slots in the sample container support 12 shown in the Figure, rotatable movement of the support 12 serves to position any container Tc, To carried in a slot 16S in the inner concentric annular array 16A to at least either a first predetermined inner sample extracting position 18I or a second predetermined inner sample extracting position 20I. Similarly, movement of the support 12 by the actuator AS serves to position any container Tc,
    To carried in a slot 16S in the outer concentric annular array 16B to at least either a first predetermined outer sample extracting position 18E or a second predetermined outer sample extracting position 20E. The sample extracting positions 18I, 18E, respectively, and the sample extracting positions 20I, 20E, respectively, are angularly offset from each other by predetermined angular distances.
  • If desired each tray 16 may have one or more arcuate row(s) of sample container receiving slots disposed between the radially inner and outer rows shown in the Figure. Such additional arcuate rows would cooperate to define additional intermediate concentric annular array(s) of slots. In accordance with this invention a pair of predetermined sample extracting positions is defined for each additional annular array. A slot in each additional annular array may be positioned at either sample extracting position in the pair by movement of the support 12.
  • In general, when a container Tc, To in a slot 16S in any particular annular array (e. g., 16A, 16B)is positioned at either of the inner sample extracting positions 18I, 20I or at either of the outer sample extracting positions 18E, 20E corresponding to that array, the liquid therein is able to be withdrawn therefrom.
  • The instrument 10 also includes a carrier 24 having a plurality of liquid receiving wells 24W therein formed to define at least one generally annular array 26. However, more preferably, the carrier 24 has at least both an inner and an outer concentric annular array 26A, 26B, respectively, of wells 24W. Each well 24W is sized to accommodate at least a predetermined liquid volume, and thus defines a receptacle wherein sample liquid may be handled and treated. The carrier 24 is operatively connected to a suitable actuator (diagrammatically indicated by the reference character Ac, similar to the actuator AS) whereby the carrier 24 is movable with respect to an axis 24A. The axis 24A is displaced from the axis 12A of the container support 12. Preferably the carrier 24 is rotatably moved with respect to the axis 24A. However, as in the case of the support 12, the carrier 24 may be otherwise movable, as in one or more rectilinear directions, some of which may be mutually perpendicular. In general the carrier 24 is movable with respect to the axis 24A to dispose any of the wells 24W at one or more predetermined positions. Preferably appropriate rotatable movement of the carrier 24 with respect to the axis 24A serves to dispose any one of the wells 24W in each annular array to at least two predetermined operating positions defined at predetermined spaced angular locations with respect to the axis 24A. It should also be noted that the wells 24W may also be otherwise arrayed, e.g., in a spiral pattern. Although shown as circular in shape in the Figure, it should be understood that the carrier 24 may exhibit any desired shape.
  • In connection with the apparatus illustrated in the Figure rotatable movement of the carrier 24 serves to position any well 24W disposed in the inner concentric circular array 26A to at least either a first predetermined inner operating position 28I or an angularly offset second predetermined inner operating position 30I. Similarly, movement of the carrier 24 by the actuator Ac serves to position any well 24W disposed in the outer concentric circular array 26B to at least either a first predetermined outer operating position 28E or an angularly offset second predetermined outer operating position 30E. If desired the carrier 24 may have one or more additional annular array(s) of wells disposed between the radially inner and outer arrays of wells shown in the Figure. At least two predetermined operating positions are defined for a well in each additional annular array of wells. As will be developed when a well 24W is disposed at a given operating position a liquid may be either drawn therefrom (i. e., extracted therefrom) and/or dispensed thereinto.
  • The instrument 10 further includes sample handling devices in the form of a first, gross, probe 40 and a second, fine, probe 50. The gross probe 40 is operatively connected to an actuator (diagrammatically indicated by the reference character Ag) whereby the probe 40 is movable along a predetermined, preferably circular, locus 42 centered about an axis 40A. The axis 40A is spaced with respect to the axes 12A and 24A of the support 12 and the carrier 24, respectively. Again, preferably the actuator Ag is implemented in the form of a belt driven by an encoded stepping motor. Similarly, the fine probe 50 is operatively connected to an actuator (diagrammatically indicated by the reference character Af, similar to the actuator Ag) whereby the probe 50 is movable along a separate predetermined locus 52. The locus 52 is centered about an axis 50A that is spaced with respect to the axes 12A and 24A of the support 12 and the carrier 24, respectively, and with respect to the axis 40A of the probe 40. The locus 52 of the fine probe 50 is also preferably generally circular in form.
  • The gross probe 40 may be implemented by any suitable liquid extracting arrangement so long as the probe 40 is able to draw (i. e., extract) liquid from either a closed or an open tube or other liquid reservoir or liquid receptacle. To satisfy the needs of the present invention the gross probe 40 is required only to be able to control in a relatively gross manner the volume of liquid able to be either drawn thereinto or dispensed therefrom. The term "relatively gross control" should be construed to mean liquid volume control to the order of ten microliters. Details of the preferred form of the liquid extraction apparatus used to implement the gross probe are disclosed and claimed in above referenced contemporaneously filed copending application, assigned to the assignee of this invention. On the other hand, the fine probe 50 is required to be able to draw or to dispense relatively finely metered amounts of liquid. The term "relatively finely metered" should be construed to mean liquid volume control to the order of tenths of microliters.
  • The locus 42 of the gross probe 40 contains the first predetermined inner sample extracting position 18I, the first predetermined outer sample extracting position 18E, the first predetermined inner operating position 28I, and the first predetermined outer operating position 28E. When positioned at either the inner sample extracting position 18I or the outer sample extracting position 18E the gross probe is able to draw thereinto liquid sample that is carried within either a closed container Tc or an open container To that is disposed by the support 12 at that sample extracting position. Moreover, when positioned at either the inner operating position 28I or the outer operating position 28E the gross probe is able either to dispense into the well 24W positioned at the position 28I, 28E liquid that has been previously drawn into the probe or to draw into the probe (i. e., extract from the well) liquid that is present in the well.
  • The locus 52 of the fine probe 50 contains the first predetermined inner sample extracting position 20I, the first predetermined outer sample extracting position 20E, the first predetermined inner operating position 30I, and the first predetermined outer operating position 30E. When positioned at either the inner sample extracting position 20I or the outer sample extracting position 20E the fine probe 50 is able to draw thereinto liquid sample that is carried within an open container To that is disposed by the support 12 at that sample extracting position. However, when positioned at either the inner operating position 30I or the outer operating position 30E the fine probe is able either to dispense into the well positioned at the position 30I, 30E liquid that has been previously drawn into the probe or to draw into the fine probe (i. e., extract from the well) liquid that is present in the well.
  • Various other liquid handling, sample analysis and/or sample treatment functional devices of the analysis instrument 10 may be positioned about the locus 42 defined by the movement of the gross probe 42. In the Figure three such representative additional devices 56, 58, 60 are respectively located at predetermined angular positions 62, 64, 66 along the locus 42. In general, each of these angular positions 62, 64, 66 defines an operating position at which the gross probe is able either to dispense liquid or to extract liquid. Of course, the precise function of the device 56, 58, 60 at each respective angular position 62, 64, 66 will serve to determine the primary action performed by the probe at a given location.
  • For example, the device 56 located at the angular position 62 is, in the preferred implementation of the instrument 10, an analysis device of the ion selective electrode (ISE) type. Suitable for use as the ion selective electrode analysis device is that device manufactured by the Medical Products division of E. I. du Pont de Nemours and Company as sold as part of the clinical chemistry system identified by the trademark Dimension®. This analysis device is disclosed in United States Patent 5,284,568 issued on February 8, 1994 and assigned to the assignee of the present invention. The primary action of the probe 40 at the analysis device 56 is the dispensation of liquid sample or treated sample from the probe into the analysis device. Accordingly, the angular location 62 serves to define a second dispensing position along the locus 42 at which the probe 40 may dispense liquid.
  • By way of further example, the device 58 located at the angular position 64 is, in the preferred implementation of the instrument 10, a liquid reservoir for either a treatment liquid, (e. g., a diluent liquid solution for diluting a patient sample or a chemical reagent for chemically treating the patient sample) or a wash station for cleaning the liquid handling probe. In the former case (diluent or reagent) the primary action of the probe 50 at the device 58 is extracting liquid from the reservoir into the probe. Accordingly, the angular location 62 would serve to define a second liquid extracting position along the locus 42 at which the probe may draw a liquid thereinto. Alternatively, in the latter case (i. e., a wash station) the device 58 disposed in the position 64 may be either a reservoir or a drain, dependent upon the form of probe wash utilized. If the wash liquid is disposed in a reservoir, then the primary actions of the probe 50 at the device 58 would include both dispensing liquid to and extracting liquid from the reservoir. However, if the wash liquid is pumped into and through the probe from a source (not shown) then the primary action of the probe 50 at the device 58 would be the dispensing of liquid into the drain. Thus at the wash location the probe 50 may either extract, dispense, or both, as appropriate.
  • It should be appreciated that if either a diluent or a reagent liquid solution is disposed in the reservoir 58, then it lies within the contemplation of the invention to dispose the wash solution in a second reservoir device 60 which may be disposed at the angular position 66. Since at a wash position the probe both dispenses and extracts, the angular position 66 would serve to define a third extracting position at which the probe 40 draws liquid thereinto. Furthermore, it should be understood that additional liquid handling, sample analysis and/or sample treatment functional devices, such as additional reservoir(s) for other chemical liquids may also be positioned at additional location(s) about the locus 42, e.g., a reservoir 58A at an angular position 64A may contain a liquid chemical reagent.
  • In similar fashion it should be understood that various additional functional devices of the analysis instrument 10 may be positioned about the locus 52 defined by the movement of the fine probe 50. In the Figure two such additional devices 70, 72 are respectively located at respective predetermined angular positions 74, 76 along the locus 52. In general, each of these angular positions 74, 76 defines an operating position at which the gross probe is able either to dispense liquid or to extract liquid. Of course, the precise function of the device 70, 72 at the respective angular position 74, 76 will serve to determine the primary action performed by the probe 50 at a given location.
  • For example, the device 70 located at the angular position 74 is, in the preferred implementation of the instrument 10, an analysis device of the photometric type. Suitable for use as the photometric analysis device is that manufactured and sold by the Medical Products division of E. I. du Pont de Nemours and Company as part of the clinical chemistry system identified by the trademark Dimension®. This photometric analysis is disclosed in United States Patent 4,863,693 issued on September 5, 1989 to G. W. Howell and assigned to the assignee of the present invention. The primary action of the probe 50 at the analysis device 70 is the dispensation of liquid from the probe into the analysis device. Accordingly, with respect to the fine probe 50, the angular location 74 serves to define a second dispensing position along the locus 52 at which the probe 50 may dispense liquid.
  • Further, the device 72 located at the angular position 76 is, in the preferred implementation of the instrument 10, a liquid reservoir, primarily for a wash solution. Noting that at a wash position the probe 50 both dispenses and extracts liquid, the angular position 76 serves to define a second liquid extracting position along the locus 52 of the probe 50. In keeping with the foregoing it should be appreciated that additional devices of various functionality may be additionally disposed at spaced angular positions along the locus 52.
  • In general, the foregoing should also make apparent that however the various analysis, treatment and/or handling devices are arranged, in accordance with the present invention both the probe 40 and the probe 50 are each independently movable along their respective loci of action 42, 52 among one or more various extracting position(s), one or more various dispensing position(s) and/or one or more various operating position(s) (i. e., both extracting and dispensing). The flexibility of operation imparted to an instrument 10 so configured may be made more clear from the following operational examples.
    • EXAMPLES
  • Three closed containers are positioned in slots 16S1, 16S2 and 16S6, the containers indicated by reference characters Tc1, Tc2 and Tc6, respectively. Three open containers are positioned in slots 16S3, 16S4 and 16S5, the containers indicated by reference characters To3, To4, To5, respectively. Slots 16S1 and 16S3 are located on the outcr concentric circular array 16B. Slots 16S2 and 16S4 are located on the inner concentric circular array 16A, respectively. Slots 16S5 and 16S6 are located on the outer concentric circular array 16B. Various different analytical tests are to be performed upon the different sample fluids contained in the different closed and open containers Tc1, Tc2, To3, To4, To5, and To6, as described below:
    • Example 1
  • Analytical Test 1 in which a liquid sample is extracted from a closed container and provided to two separate analysis devices without pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S1 containing closed container Tc1 at a first predetermined outer sample extracting position 18E. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined outer sample extracting position 18E and is operated to extract a first predetermined sample volume from closed container Tc1. Gross probe 40 is withdrawn from the sample volume, operated to extract a volume of air and repositioned to extract a second predetermined sample volume from closed container Tc1, the volume of air separating the first and second predetermined sample volumes.
  • 2. Carrier 24 is rotated by actuator Ac to position well 26W1 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the second predetermined sample volume taken previously from closed container Tc1 is disposed into well 24W1. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the second dispensing position located at angular position 62 along the locus 42 whereat the first predetermined sample volume taken previously from closed container Tc1 is disposed into an analysis instrument 56 located at the second dispensing position.
  • 3. Carrier 24 is next rotated by actuator Ac to position well 24W1 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the second predetermined sample volume taken previously from closed container Tc1 and disposed into well 24W1 by gross probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the second predetermined sample volume taken previously from closed container Tc1 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
    • Example 2
  • Analytical test 2 in which liquid sample is extracted from a closed container and provided to a first analysis device without pretreatment and is also provided to a second analysis device after a diluting pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S2 containing container Tc2 at the first predetermined inner sample extracting position 18I. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined inner sample extracting position 18I and is operated to extract a first predetermined sample volume from closed container Tc2. Gross probe 40 is withdrawn from the sample volume, operated to extract a volume of air and repositioned to extract a second predetermined sample volume from closed container Tc2, the volume of air separating the first and second predetermined sample volumes.
  • 2. Carrier 24 is rotated by actuator Ac to position well 24W2 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the second predetermined sample volume taken previously from closed container Tc1 is disposed into well 26W2. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the second dispensing position located at angular position 62 along the locus 42 whereat the first predetermined sample volume taken previously from closed container Tc1 is disposed into an analysis instrument 56 located at the second dispensing position.
  • 3. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 66 along the locus 42 whereat a wash solution is disposed in the second device 60. Gross probe is operated to extract wash solution thereinto and subsequently to extract wash solution therefrom, a process that may be repeated sufficiently to cleanse gross probe 40.
  • 4. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 64 along the locus 42 whereat a dilution solution is disposed in the device 58. Gross probe 40 is next operated to extract a predetermined volume of dilution solution therefrom. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the predetermined volume of dilution solution taken previously from device 58 is disposed into well 24W2.
  • 5. Carrier 24 is next rotated by actuator Ac to position well 24W2 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the second predetermined sample volume taken previously from closed container Tc2 and the predetermined volume of dilution solution taken previously from device 58 and also disposed into well 24W2 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second operating position 30I whereat the second predetermined sample volume taken previously from closed container Tc2 and the predetermined volume of dilution solution taken previously from device 58 and also disposed into well 24W2 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
    • Example 3
  • Analytical Test 3 in which a liquid sample is extracted from an open container and provided to two separate analysis instruments without pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S3 containing open container To3 at the first predetermined outer sample extracting position 18E. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined outer sample extracting position 18E. Gross probe 40 is operated to extract a first predetermined sample volume from open container To3, is withdrawn from the liquid sample, operated to extract a volume of air, and repositioned into the liquid to extract a second predetermined sample volume from open container To3, the volume of air separating the first and second predetermined sample volumes.
  • 2. Carrier 24 is rotated by actuator Ac to position well 24W3 in the outer concentric annular array of wells 26B at the first predetermined outer operating position 28E. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined outer operating position 28E whereat the second predetermined sample volume taken previously from open container To3 is disposed into well 24W3. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the second dispensing position located at angular position 62 along the locus 42 whereat the first predetermined sample volume taken previously from open container To3 is disposed into an analysis instrument 56 located at the second dispensing position.
  • 3. Carrier 24 is next rotated by actuator Ac to position well 24W3 in the outer concentric annular array of wells 26B at the second predetermined outer operating position 30E. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second predetermined outer operating position 30E whereat the second predetermined sample volume taken previously from open container To3 and disposed into well 24W3 by gorss probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the second predetermined sample volume taken previously from open container To3 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
    • Example 4
  • Analytical Test 4 in which a liquid sample is extracted from a closed container and provided to a first analysis device after pretreatment and is also provided to a second analysis device before and after a diluting pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S6 containing closed container Tc6 at the first predetermined outer sample extracting position 18E. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined sample outer extracting position 18E. Gross probe 40 is operated to extract a first predetermined sample volume from closed container Tc6, is withdrawn from the sample liquid operated to extract a first volume of air and repositioned into the sample liquid to extract a second predetermined sample volume from closed container Tc6, operated to extract a second volume of air and repositioned to extract a third predetermined sample volume from closed container Tc6, the first and second volumes of air separating the first, second and third predetermined sample volumes.
  • 2. Carrier 24 is rotated by actuator Ac to position well 24W6 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the third predetermined sample volume taken previously from closed container Tc6 is disposed into well 24W6.
  • 3. Carrier 24 is rotated by actuator Ac to position well 24W7 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the second predetermined sample volume taken previously from closed container Tc6 is disposed into well 24W7.
  • 4. Carrier 24 is rotated by actuator Ac to position well 24W4 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the first predetermined sample volume taken previously from closed container Tc6 is disposed into well 24W4.
  • 5. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 66 along the locus 42 whereat a wash solution is disposed in the second device 60. Gross probe 40 is operated to extract wash solution thereinto and subsequently to extract wash solution therefrom, a process that may be repeated sufficiently to cleanse gross probe 40.
  • 6. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 64 along the locus 42 whereat a dilution solution is disposed in the device 58. Gross probe is next operated to extract a predetermined volume of dilution solution therefrom. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat a predetermined portion of dilution solution taken previously from device 58 is disposed into well 24W6 and whereat a predetermined portion of dilution solution taken previously from device 58 is disposed into well 24W4.
  • 7. Carrier 24 is next rotated by actuator Ac to position well 24W6 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the third predetermined sample volume taken previously from closed container Tc6 and disposed into well 24W6 by gross probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the third predetermined sample volume taken previously from closed container Tc6 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
  • 8. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at angular position 76 along the locus 52 whereat a wash solution is disposed in an additional device 72. Fine probe is operated to extract wash solution thereinto and subsequently to extract wash solution therefrom, a process that may be repeated sufficiently to cleanse fine probe 50.
  • 9. Carrier 24 is next rotated by actuator Ac to position well 24W7 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the second predetermined sample volume taken previously from closed container Tc6 and the predetermined volume of dilution solution taken previously from device 58 and also disposed into well 24W7 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second dispensing position whereat the second predetermined sample volume taken previously from closed container Tc6 and the predetermined volume of dilution solution take previously from device 58 and also disposed into well 24W7 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
  • 10. Carrier 24 is next rotated by actuator Ac to position well 26W4 in the inner concentric annular array of wells 24A at the second predetermined inner operating position 30I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the predetermined portion of dilution solution taken previously from device 58 is disposed into well 24W4 and whereat the predetermined portion of dilution solution taken previously from device 58 is disposed into well 24W4 are extracted therefrom. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the second dispensing position located at angular position 62 along the locus 42 whereat the first predetermined sample volume taken previously from closed container Tc6 and the predetermined portion of dilution solution taken previously from device 58 are dispensed.
    • Example 5
  • Analytical Test 5 in which a first liquid sample is extracted from an open container and provided directly to a first analysis device without pretreatment and in which a second liquid sample is extracted from an open container and provided directly to a second analysis device without pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S4 containing open container To4 at the first predetermined inner sample extracting position 18I. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined inner extracting position 18I. Gross probe 40 is operated to extract a first predetermined sample volume from open container To4.
  • 2. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the second dispensing position located at angular position 62 along the locus 42 whereat the first predetermined sample volume taken previously from open container To4 is disposed into an analysis instrument 56 located at the second dispensing position.
  • 3. Support 12 is rotated by actuator As to position slot 16S4 containing open container To4 at the second predetermined inner sample extracting position 20I. Fine probe 50 is rotated by actuator Af to position fine probe 50 at the second predetermined inner sample extracting position 20I and is operated to extract a second predetermined sample volume from open container To4. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second predetermined dispensing position whereat the second predetermined sample volume previously taken from open container To4 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
    • Example 6
  • Analytical Test 6 in which liquid samples extracted from closed and open containers are provided to an analysis device(s) in a different sequence than that in which they were extracted from the containers without pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S1 containing closed container Tc1 at a first predetermined outer sample extracting position 18E. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined outer sample extracting position 18E and is operated to extract a first predetermined sample volume from closed container Tc1.
  • 2. Carrier 24 is rotated by actuator Ac to position well 24W1 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the first predetermined sample volume taken previously from closed container Tc1 is disposed into well 24W1.
  • 3. Support 12 is rotated by actuator As to position slot 16S2 containing closed container Tc2 at a first predetermined inner sample extracting position 18I. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined inner extracting position 18I and is operated to extract a second predetermined sample volume from closed container Tc2.
  • 4. Carrier 24 is rotated by actuator Ac to position well 24W2 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the second predetermined inner operating position 281 whereat the second predetermined sample volume taken previously from closed container Tc2 is disposed into well 24W2.
  • 5. Support 12 is rotated by actuator As to position slot 16S3 containing open container To3 at a first predetermined outer sample extracting position 18E. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined outer sample extracting position 18E and is operated to extract a third predetermined sample volume from open container To3.
  • 6. Carrier 24 is rotated by actuator Ac to position well 24W3 in the outer concentric annular array of wells 26A at the first predetermined outer operating position 28E. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined outer operating position 28E whereat the third predetermined sample volume taken previously from open container To3 is disposed into well 24W3.
  • 7. Support 12 is rotated by actuator As to position slot 16S4 containing open container To4 at a first predetermined inner sample extracting position 18I. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined inner extracting position 18I and is operated to extract a fourth predetermined sample volume from open container To4.
  • 8. Carrier 24 is rotated by actuator Ac to position well 24W4 in the inner concentric annular array of wells 24A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the fourth predetermined sample volume taken previously from open container To4 is disposed into well 24W4.
  • 9. Carrier 24 is next rotated by actuator Ac to position well 24W2 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the second predetermined sample volume taken previously from closed container Tc2 and disposed into well 24W2 by gross probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the second predetermined sample volume taken previously from closed container Tc2 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
  • 10. Carrier 24 is next rotated by actuator Ac to position well 24W4 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the first predetermined sample volume taken previously from open container To4 and disposed into well 24W4 by gross probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the fourth predetermined sample volume taken previously from open container To4 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
  • 11. Carrier 24 is next rotated by actuator Ac to position well 24W1 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the first predetermined sample volume taken previously from closed container Tc1 and disposed into well 24W1 by gross probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the first predetermined sample volume taken previously from closed container Tc1 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
  • 12. Carrier 24 is next rotated by actuator Ac to position well 24W3 in the outer concentric annular array of wells 26B at the second predetermined outer operating position 30E. Fine probe 50 is rotated by actuator Af to position fine probe 50 at the second predetermined outer operating position 30E whereat the third predetermined sample volume taken previously from open container To3 and disposed into well 24W3 by gross probe 40 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to angular position 74 along the locus 52 whereat the third predetermined sample volume taken previously from open container To3 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
    • Example 7
  • Analytical Test 7 in which a liquid sample is extracted from a closed container and provided to a second analysis device after a diluting pretreatment and after a chemical reagent pretreatment.
  • 1. Support 12 is rotated by actuator As to position slot 16S2 containing closed container Tc2 at the first predetermined inner sample extracting position 18I. Gross probe 40 is rotated by actuator Ag to position gross probe 40 at the first predetermined inner sample extracting position 18I and is operated to extract a first predetermined sample volume from closed container Tc2.
  • 2. Carrier 24 is rotated by actuator Ac to position well 24W2 in the inner concentric annular array of wells 26A at the first predetermined inner operating position 28I. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the first predetermined sample volume taken previously from closed container Tc1 is disposed into well 24W2.
  • 3. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 66 along the locus 42 whereat a wash solution is disposed in the second device 60. Gross probe 40 is operated to extract wash solution thereinto and subsequently to extract wash solution therefrom, a process that may be repeated sufficiently to cleanse gross probe 40.
  • 4. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 64 along the locus 42 whereat a dilution solution is disposed in the device 58. Gross probe 40 is next operated to extract a predetermined volume of dilution solution therefrom. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the predetermined volume of dilution solution taken previously from device 58 is disposed into well 24W2.
  • 5. Gross probe 40 is next rotated by acutator Ag to position gross probe 40 at angular position 66 along the locus 42 whereat a wash solution is disposed in the second device 60. Gross probe 40 is operated to extract wash solution thereinto and subsequently to extract wash solution therefrom, a process that may be repeated sufficiently to cleanse gross probe 40.
  • 6. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at angular position 64A along the locus 42 whereat a chemical reagent solution is disposed in the device 58A. Gross probe is next operated to extract a predetermined volume of chemical reagent solution therefrom. Gross probe 40 is next rotated by actuator Ag to position gross probe 40 at the first predetermined inner operating position 28I whereat the predetermined volume of chemical reagent taken previously from device 58A is disposed into well 24W2. At this point, if desired, a predetermined period of time may be allowed to elapse before the following step 7 is enacted.
  • 7. Carrier 24 is next rotated by actuator Ac to position well 24W2 in the inner concentric annular array of wells 26A at the second predetermined inner operating position 30I. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second predetermined inner operating position 30I whereat the first predetermined sample volume taken previously from closed container Tc2 and the predetermined volume of dilution solution taken previously from device 58 and the predetermined volume of chemical reagent taken previously from device 58A and also disposed into well 24W2 is extracted therefrom. Fine probe 50 is next rotated by actuator Af to position fine probe 50 at the second dispensing position 74 whereat the first predetermined sample volume taken previously from closed container Tc2 and the predetermined volume of dilution solution taken previously from device 58 and the predetermined volume of chemical reagent taken previously from device 58A and also disposed into well 24W2 is disposed by fine probe 50 into an analysis device 70 located at the second dispensing position.
  • Those skilled in the art, having the benefit of the teachings of the present invention may effect numerous modifications thereo. Such modifications are to be construed as lying within the contemplation of the present invention, as defined by the appended claims.

Claims (3)

  1. An apparatus comprising:
    a support (12) for supporting closed or open containers (Tc,To), the support (12) being movable with respect to an axis (12A) to dispose any one of the containers (Tc,To) at a gross probe sample extracting position (18I,18E) and at a fine probe sample extracting position (20I,20E),
    a gross probe (40) movable along a locus of action (42) between the gross probe sample extracting position (18I,18E) and a gross probe sample dispensing position (28I,28E), in the gross probe sample extracting position (18I,18E) the gross probe (40) being able to draw thereinto liquid from either a closed or an open container (Tc,To) disposed by the support (12) at the gross probe sample extracting position (18I,18E), in the gross probe dispensing position (28I,28E) the gross probe being able to dispense therefrom previously withdrawn liquid,
    a fine probe (50) movable along a locus of action (42) between the fine probe sample extracting position (20I,20E) and a fine probe operating position (30I,30E), in the fine probe sample extracting position (20I,20E) the fine probe (50) being able to draw thereinto liquid from an open container (To) disposed by the support (12) at the fine probe sample extracting position (20I,20E), in the fine probe operating position (30I,30E) the fine probe being able either to dispense therefrom previously withdrawn liquid or to draw thereinto liquid, and
    a carrier (24) having a plurality of liquid receiving wells (24W) therein, the carrier (24) being movable with respect to an axis (24A) spaced from the axis (12A) of the support (12) to dispose any one of the plurality of wells (24W) therein at either the gross probe dispensing position (28I,28E) or the fine probe operating position (30I,30E), the well (24W) disposed at the gross probe dispensing position (28I,28E) being able to receive liquid dispensed from the gross probe (40), the well (24W) disposed at the fine probe operating position (30I,30E) being able to receive liquid dispensed thereinto from the fine probe or have liquid drawn therefrom by the fine probe.
  2. Apparatus according to claim 1, further comprising:
    a liquid analysis device (70) located at the fine probe dispensing position (74),
    the fine probe (50) also being movable along the locus of action (52) to the fine probe dispensing position (74),
    at the fine probe dispensing position (74) the fine probe (50) being able to dispense therefrom previously withdrawn liquid to the liquid analysis device (70).
  3. Apparatus according to claim 1, wherein
    the plurality of containers (Tc,To) on the support (12) being arranged in at least an inner and an outer concentric annular array, the support (12) being movable to dispose any one of the containers (Tc,To) in the inner concentric annular array (16A) at either an inner gross probe sample extracting position (18I) or at an inner fine probe sample extracting position (20I) and any one of the containers (Tc,To) in the outer concentric annular array (16A) at either an outer gross probe sample extracting position (18E) or at an outer fine probe sample extracting position (20E), and wherein
    the plurality of liquid receiving wells (24W) on the carrier (24) being arranged in at least an inner and an outer concentric annular array (26A,26B), the support (12) being movable to dispose any one of the wells (24W) in the inner concentric annular array (26A) at either an inner gross probe operating position (28I) or at an inner fine probe operating position (30I) and any one of the wells (24W) in the outer concentric annular array (26B) at either an outer gross probe operating position (28E) or at an outer fine probe operating position (30E).
EP95110802A 1994-07-15 1995-07-11 Analysis instrument Expired - Lifetime EP0692717B1 (en)

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US276186 1988-11-23
US27618694A 1994-07-15 1994-07-15

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EP0692717A2 EP0692717A2 (en) 1996-01-17
EP0692717A3 EP0692717A3 (en) 1997-01-08
EP0692717B1 true EP0692717B1 (en) 2000-03-15

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JP (1) JPH0854382A (en)
DE (1) DE69515565T2 (en)

Families Citing this family (17)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JP3032159B2 (en) * 1996-09-24 2000-04-10 株式会社日立製作所 Analysis system
EP1058118B1 (en) * 1999-06-04 2013-02-27 Randox Laboratories Ltd. Liquid dispenser on mobile support
JP3972012B2 (en) * 2003-03-19 2007-09-05 株式会社日立ハイテクノロジーズ Sample dispensing mechanism and automatic analyzer equipped with the same
US7381370B2 (en) * 2003-07-18 2008-06-03 Dade Behring Inc. Automated multi-detector analyzer
US8133115B2 (en) * 2003-10-22 2012-03-13 Sony Computer Entertainment America Llc System and method for recording and displaying a graphical path in a video game
US20060071933A1 (en) 2004-10-06 2006-04-06 Sony Computer Entertainment Inc. Application binary interface for multi-pass shaders
US7636126B2 (en) * 2005-06-22 2009-12-22 Sony Computer Entertainment Inc. Delay matching in audio/video systems
US7880746B2 (en) * 2006-05-04 2011-02-01 Sony Computer Entertainment Inc. Bandwidth management through lighting control of a user environment via a display device
US7965859B2 (en) 2006-05-04 2011-06-21 Sony Computer Entertainment Inc. Lighting control of a user environment via a display device
US10786736B2 (en) 2010-05-11 2020-09-29 Sony Interactive Entertainment LLC Placement of user information in a game space
TWI527565B (en) * 2010-07-08 2016-04-01 賽諾菲阿凡提斯德意志有限公司 Allowing measurements to be made of a blood sample
CN103376333B (en) * 2012-04-17 2015-09-16 深圳迈瑞生物医疗电子股份有限公司 Automatic clinical chemistry analyzer
ES2901756T3 (en) 2013-03-15 2022-03-23 Abbott Lab Automated diagnostic analyzers having rear accessible track systems and related methods
JP6165961B2 (en) 2013-03-15 2017-07-19 アボット・ラボラトリーズAbbott Laboratories Diagnostic analyzer with pre-process carousel and associated method
US9400285B2 (en) 2013-03-15 2016-07-26 Abbot Laboratories Automated diagnostic analyzers having vertically arranged carousels and related methods
JP6521567B2 (en) * 2014-02-27 2019-05-29 キヤノンメディカルシステムズ株式会社 Clinical examination equipment
US10094842B2 (en) 2014-10-17 2018-10-09 Shenzhen Mindray Bio-Medical Electronics Co., Ltd. Automatic biochemical analyzer

Family Cites Families (40)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3497320A (en) * 1966-12-15 1970-02-24 Xerox Corp Automated chemical analyzer
US3552441A (en) * 1967-09-26 1971-01-05 Hartmut Luhleich Piercable closure diaphragm for a chamber
FR2120300A5 (en) * 1970-12-29 1972-08-18 Hoffmann La Roche
JPS5782769A (en) * 1980-11-10 1982-05-24 Hitachi Ltd Automatic analyzing device
US4622457A (en) * 1981-03-09 1986-11-11 Spectra-Physics, Inc. Autosampler mechanism
JPS5810657A (en) * 1981-07-13 1983-01-21 Toshiba Corp Automatic chemical analyzer
DE3229118A1 (en) * 1981-08-05 1983-03-24 Varian Techtron Proprietary Ltd., 3170 Mulgrave, Victoria DEVICE FOR HANDLING SAMPLES
JPS5985959A (en) * 1982-11-09 1984-05-18 Nippon Tectron Co Ltd Automatic analyzing apparatus
US4622475A (en) 1984-03-05 1986-11-11 Tektronix, Inc. Data storage element having input and output ports isolated from regenerative circuit
US4577514A (en) 1984-04-09 1986-03-25 Vanderbilt University Method and apparatus for sampling liquid phase components from a liquid-semisolid fluid
US4761268A (en) * 1984-04-12 1988-08-02 Fisher Scientific Company Liquid handling
US4863693A (en) 1984-08-21 1989-09-05 E. I. Du Pont De Nemours And Company Analysis instrument having a blow molded reaction chamber
US4729876A (en) * 1984-11-27 1988-03-08 Nova Celltrak, Inc. Blood analysis system
JPS61274268A (en) * 1985-05-30 1986-12-04 Toshiba Corp Automatic chemical analyzer
JPH0786509B2 (en) * 1985-06-18 1995-09-20 株式会社東芝 Automatic chemical analyzer
EP0216026B1 (en) 1985-06-26 1992-01-22 Japan Tectron Instruments Corporation Automatic analysis apparatus
US4756201A (en) 1985-09-03 1988-07-12 Technicon Instruments Corporation Apparatus and method for combined closed and open tube sampling
JPH0692975B2 (en) * 1985-09-11 1994-11-16 株式会社東芝 Automatic chemical analyzer
EP0221315B1 (en) 1985-10-09 1989-06-14 Kontron Instruments Holding N.V. Liquid-withdrawing device
JPH0690212B2 (en) * 1986-02-21 1994-11-14 株式会社東芝 Automatic chemical analyzer
JPH0754326B2 (en) * 1986-06-24 1995-06-07 株式会社東芝 Automatic chemical analyzer
DE3783521T2 (en) * 1986-07-11 1993-05-13 Beckman Instruments Inc MODULAR ANALYSIS SYSTEM.
US5212094A (en) * 1986-09-16 1993-05-18 Kabushiki Kaisha Toshiba Automatic chemical analyzer
JPH06103315B2 (en) * 1987-08-14 1994-12-14 株式会社東芝 Dispensing nozzle device of automatic chemical analyzer
JP2708437B2 (en) * 1987-11-13 1998-02-04 株式会社日立製作所 Automatic analyzer
US5051238A (en) * 1987-11-20 1991-09-24 Hitachi, Ltd. Automatic analyzing system
US4836038A (en) * 1988-03-18 1989-06-06 Aim Instruments Ltd. Automated sampler-injector apparatus and method for sampling a quantity of sample and testing portions of said quantity
US4951512A (en) 1988-06-23 1990-08-28 Baxter International Inc. System for providing access to sealed containers
US5104808A (en) * 1988-08-26 1992-04-14 Laska Paul F Method and apparatus for effecting a plurality of assays on a plurality of samples in an automatic analytical device
WO1990008307A1 (en) 1988-12-29 1990-07-26 Technicon Instruments Corporation Integrated sampler for closed and open sample containers
JP2539512B2 (en) * 1989-07-17 1996-10-02 株式会社日立製作所 Multi-item analyzer and method for operating the analyzer
US5209903A (en) * 1989-09-06 1993-05-11 Toa Medical Electronics, Co., Ltd. Synthetic apparatus for inspection of blood
US5216926A (en) * 1990-04-18 1993-06-08 E. I. Du Pont De Nemours And Company Closed and open tube sampling apparatus
US5080864A (en) * 1990-07-20 1992-01-14 Eastman Kodak Company Stopper detector
CA2046813A1 (en) * 1990-10-02 1992-04-03 Ueli Stettler Apparatus for introducing pipetting inserts through sample cup closures
US5128103A (en) * 1990-12-14 1992-07-07 E. I. Du Pont De Nemours And Company Apparatus for automatically processing magnetic solid phase reagents
DE4121089A1 (en) * 1991-06-26 1993-01-07 Boehringer Mannheim Gmbh ANALYSIS SYSTEM FOR THE AUTOMATIC ANALYSIS OF BODY LIQUIDS
US5376313A (en) * 1992-03-27 1994-12-27 Abbott Laboratories Injection molding a plastic assay cuvette having low birefringence
US5296911A (en) * 1992-07-16 1994-03-22 Schiapparelli Biosystems, Inc. Optical test system for a chemical analyzer
US5270211A (en) * 1992-07-16 1993-12-14 Schiapparelli Biosystems, Inc. Sample tube entry port for a chemical analyzer

Also Published As

Publication number Publication date
US5717148A (en) 1998-02-10
JPH0854382A (en) 1996-02-27
EP0692717A3 (en) 1997-01-08
EP0692717A2 (en) 1996-01-17
DE69515565D1 (en) 2000-04-20
DE69515565T2 (en) 2000-11-02

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